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Human IgM xenoreactive natural antibodies can induce resistance of porcine endothelial cells to complement-mediated injury
Authors:Agustin R Dalmasso  Tao He  Barbara A. Benson
Affiliation:Pathology and Laboratory Medicine Service, Department of Veterans Affairs Medical Center, and University of Minnesota, Minneapolis, Minnesota
Abstract:Abstract: It is thought that human IgM xenoreactive natural antibodies (nAbs) can induce activation of porcine endothelial cells independent of complement. Therefore we hypothesized that pretreatment of porcine endothelial cells with anti-pig nAbs may affect the ability of the endothelial cells, when subsequently incubated with a source of nAbs and complement, to bind antibodies and complement components and to undergo complement-mediated cytotoxicity. We preincubated porcine endothelial cells at 37°C for 1 hr or 40 hr with a source of nAbs. We then incubated these pretreated endothelial cells with a complement source that contained a normal complement level and a low level of IgM nAbs for 1 hr to measure bound IgM and IgG and complement components, and for 4 hr to measure cytotoxicity. We found that preincubation for as long as 40 hr did not impair the binding of IgM and IgG, implying no antibody-induced loss of membrane antigens from the endothelial cells, or the binding of C3bi, C4d, C6, and C9 upon complement activation. In contrast, preincubation for 40 hr with a nAb source induced in the endothelial cells marked resistance to complement-mediated killing. Resistance could be induced with purified human IgM but not with purified IgG or IgM-depleted human serum. The ability of purified IgM to induce resistance was abrogated by removal of anti-pig xenoreactive nAbs by absorption with pig endothelial cells, and induction of resistance required protein synthesis. We conclude that prolonged incubation of human anti-pig nAbs with pig endothelial cells does not cause loss of endothelial cell membrane antigens or impairment in binding of nAbs or complement components; instead, it induces marked resistance to complement-mediated cytotoxicity. These observations may be of value to develop strategies that enhance survival of a xenograft.
Keywords:xenoreactivity    xenotransplantation    endothelial cells    complement    natural antibodies
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